Bipolar Disorder
Conditions
Brief summary
The objective of this retrospective observational study is to compare commonly prescribed bipolar disorder medications for their impact on: (1) hospitalization; (2) suicide attempts and self-harm; and (3) risk of drug-induced adverse effects such as kidney disease and diabetes mellitus. In addition, the investigators will examine heterogeneity of treatment effect by co-morbidity within pediatric, adult, and elderly sub-populations. Patient focus groups are convened to elicit additional questions and provide feedback on results.
Detailed description
Funded by PCORI, the objective of this retrospective observational study is to perform several safety and effectiveness comparisons on commonly prescribed bipolar disorder medications, engaging patient focus groups in generating additional questions and interpreting results. The study will be a retrospective cohort study conducted with administrative claims data from the Truven MarketScan Commerical Claims and Encounters and Medicare database from 2010-2016. The database contains approximately 140 million patients within the US population in every state and nearly every county in the nation, across all ages, ethnicities and socioeconomic categories, including privately insured, and Medicare patients. The study will focus on approximately one million patients with two or more diagnoses of bipolar disorder in the claims records according to ICD-9 and/or ICD-10 coding. The treatments that will be compared are lithium carbonate; first generation antipsychotics: haloperidol and perphenazine; second generation antipsychotics: clozapine, risperidone, olanzapine, aripiprazole, quetiapine, ziprasidone, asenapine, lurasidone, and paliperidone; mood stabilizing anticonvulsants: valproate, lamotrigine, carbamazepine, and oxcarbazepine; antidepressants: mirtazapine, bupropion, desvenlafaxine, duloxetine, venlafaxine, citalopram, escitalopram, fluoxetine, fluvoxamine, paroxetine, sertraline, vilazodone, and doxepin. The investigators will perform cross-sectional and survival based analysis using regression, propensity scoring, and local control to perform bias-corrected comparisons of the above treatments for for their impact on: (1) hospitalization; (2) suicide attempts and self-harm; and (3) risk of drug-induced adverse effects such as kidney disease and diabetes mellitus. In addition, the investigators will examine heterogeneity of treatment effect by co-morbidity within pediatric, adult, and elderly sub-populations.
Interventions
DRUGQuetiapine
Exposure to all dosages and delivery forms.
DRUGOlanzapine
Exposure to all dosages and delivery forms.
DRUGAripiprazole
Exposure to all dosages and delivery forms.
DRUGFluoxetine / Olanzapine
Exposure to all dosages and delivery forms.
DRUGLithium Carbonate
Exposure to all dosages and delivery forms.
DRUGLamotrigine
Exposure to all dosages and delivery forms.
DRUGValproic Acid
Exposure to all dosages and delivery forms.
DRUGOxcarbazepine
Exposure to all dosages and delivery forms.
DRUGCarbamazepine
Exposure to all dosages and delivery forms.
DRUGZiprasidone
Exposure to all dosages and delivery forms.
DRUGRisperidone
Exposure to all dosages and delivery forms.
DRUGHaloperidol
Exposure to all dosages and delivery forms.
DRUGPerphenazine
Exposure to all dosages and delivery forms.
DRUGClozapine
Exposure to all dosages and delivery forms.
DRUGAsenapine
Exposure to all dosages and delivery forms.
DRUGLurasidone
Exposure to all dosages and delivery forms.
DRUGPaliperidone
Exposure to all dosages and delivery forms.
DRUGMirtazapine
Exposure to all dosages and delivery forms.
DRUGBupropion
Exposure to all dosages and delivery forms.
DRUGDesvenlafaxine
Exposure to all dosages and delivery forms.
DRUGDuloxetine
Exposure to all dosages and delivery forms.
DRUGVenlafaxine
Exposure to all dosages and delivery forms.
DRUGCitalopram
Exposure to all dosages and delivery forms.
DRUGEscitalopram
Exposure to all dosages and delivery forms.
DRUGFluoxetine
Exposure to all dosages and delivery forms.
DRUGFluvoxamine
Exposure to all dosages and delivery forms.
DRUGParoxetine
Exposure to all dosages and delivery forms.
DRUGSertraline
Exposure to all dosages and delivery forms.
DRUGVilazodone
Exposure to all dosages and delivery forms.
DRUGDoxepin
Exposure to all dosages and delivery forms.
Sponsors
Patient-Centered Outcomes Research Institute
Montana State University
National Alliance on Mental Illness Montana
CGStat LLC
Risk Benefit Statistics LLC
National Alliance on Mental Illness New Mexico
National Alliance on Mental Illness Westside Los Angeles
University of New Mexico
Study design
Observational model
COHORT
Time perspective
RETROSPECTIVE
Eligibility
Sex/Gender
ALL
Healthy volunteers
No
Inclusion criteria
* Two or more instances of bipolar disorder diagnoses within administrative claims records
Exclusion criteria
* Patients with less than 1 year of history in the database
Design outcomes
Primary
| Measure | Time frame | Description |
|---|---|---|
| Risk of hospitalization | 0-7 years | For each treatment, assess the risk of rehospitalization within 30-days after hospitalization for a mood episode. For each treatment, assess the cumulative incidence of hospitalization for a mood episode any time after commencing treatment, accounting for the competing risk of ending treatment. |
| Risk of suicide and self-harm | 0-7 years | For each treatment, assess the cumulative risk of a second suicide or self-harm event after diagnosis of a first event, accounting for the competing risk of ending treatment. Self-harm includes injuries of unknown intent. |
Secondary
| Measure | Time frame | Description |
|---|---|---|
| Kidney disease | 0-7 years | For each treatment, assess time to first instance of renal condition. |
| Diabetes mellitus | 0-7 years | For each treatment, assess time to diagnosis of diabetes mellitus |
Countries
United States
Outcome results
None listed